Bromide ions nucleophilicity

Hydroxide ion Methyl bromide Methyl alcohol Bromide ion (nucleophile) (substrate) (product) (leaving group)... 

The major difference between the two mechanisms is the second step The second step m the reaction of tert butyl alcohol with hydrogen chloride is the ummolecular dis sociation of tert butyloxonium ion to tert butyl cation and water Heptyloxonium ion however instead of dissociating to an unstable primary carbocation reacts differently It IS attacked by bromide ion which acts as a nucleophile We can represent the transition state for this step as... 

Bromide ion forms a bond to the primary carbon by pushing off a water molecule This step IS bimolecular because it involves both bromide and heptyloxonium ion Step 2 IS slower than the proton transfer m step 1 so it is rate determining Using Ingold s ter mmology we classify nucleophilic substitutions that have a bimolecular rate determining step by the mechanistic symbol Sn2... 

The secondary carbon bears more of the positive charge than does the primary carbon and attack by the nucleophilic bromide ion is faster there Hence the major product is the secondary bromide... 

Deprotection by this method rests on the ease with which benzyl esters are cleaved by nucleophilic attack at the benzylic carbon m the presence of strong acids Bromide ion IS the nucleophile... 

S-Alkylthiiranium salts, e.g. (46), may be desulfurized by fluoride, chloride, bromide or iodide ions (Scheme 62) (78CC630). With chloride and bromide ion considerable dealkylation of (46) occurs. In salts less hindered than (46) nucleophilic attack on a ring carbon atom is common. When (46) is treated with bromide ion, only an 18% yield of alkene is obtained (compared to 100% with iodide ion), but the yield is quantitative if the methanesulfenyl bromide is removed by reaction with cyclohexene. Iodide ion has been used most generally. Sulfuranes may be intermediates, although in only one case was NMR evidence observed. Theoretical calculations favor a sulfurane structure (e.g. 17) in the gas phase, but polar solvents are likely to favor the thiiranium salt structure. 

Halide ions may attack 5-substituted thiiranium ions at three sites the sulfur atom (Section 5.06.3.4.5), a ring carbon atom or an 5-alkyl carbon atom. In the highly sterically hindered salt (46) attack occurs only on sulfur (Scheme 62) or the S-methyl group (Scheme 89). The demethylation of (46) by bromide and chloride ion is the only example of attack on the carbon atom of the sulfur substituent in any thiiranium salt (78CC630). Iodide and fluoride ion (the latter in the presence of a crown ether) prefer to attack the sulfur atom of (46). cis-l-Methyl-2,3-di-t-butylthiiranium fluorosulfonate, despite being somewhat hindered, nevertheless is attacked at a ring carbon atom by chloride and bromide ions. The trans isomer could not be prepared its behavior to nucleophiles is therefore unknown (74JA3146). 

If the addition of Br to the alkene results in a bromonium ion, the anti stereochemistry can be readily eiqilained. Nucleophilic ring opening by bromide ion would occur by backside attack at carbon, with rupture of one of the C—Br bonds, giving overall anti addition. 

The rate-determining expulsion of bromide ion through a bridged intermediate requires an anti orientation of the two bromides. The nucleophilic attack of iodide at one bromide enhances its nucleophilicity and permits formation of the bridged ion. The stereochemical preference in noncyclic systems is also anti, as indicated by the fact that /neso-stilbene... 

There is no published mechanistic study on the Auwers flavone synthesis. The mechanism may involve the nucleophilic addition of oxonium 7, derived from 1, with hydroxide to give 8. Base-promoted ring opening of 8 could provide the putative intermediate 9, which then could undergo an intramolecular Michael addition to form 10. Expulsion of bromide ion from 10 would then give flavonol 2. 

The ortho indirect deactivating effect of the two methyl groups in 2,6-dimethyl-4-nitropyridine 1-oxide (163) necessitates a much higher temperature (about 195°, 24 hr) for nucleophilic displacement of the nitro group by chloride (12iV HCl) or bromide ions N HBr) than is required for the same reaction with 4-nitropyridine 1-oxide (110°). With 5-, 6-, or 8-methyl-4-chloroquinolines, Badey observed 2-7-fold decreases in the rate of piperidino-dechlorination relative to that of the des-methyl parent (cf. Tables VII and XI, pp. 276 and 338, respectively). 

The chemoselectivity of the other alkenes of Table 1 is more variable. It appears that bulky substituents favour bromide over methanol attack of the bromonium ion, since dibromlde increases from 39 to 70 % on going from methyl to tert-butyl in the monosubstituted series. The same trend is observed in the disubstituted series with a contraction of the chemoselectivity span (37 to 43 % on going from methyl to teH-butyl) for the trans isomers. Since the solvated bromide ion can be viewed as a nucleophile larger than methanol, the influence of steric effects, important in determining the regioselectivity, does not seem very significant as regards the chemoselectivity. This result has been interpreted in terms of a different balance between polar and steric effects of the substituents on these two selectivities. 

It has been shown (ref. 21) that a solvent which is both protic and nucleophilic, assists the formation of the bromination intermediates of moderately reactive olefins as styrenes in two ways, (Scheme 7). Firstly, the solvent initiates bromide ion formation electrophilically and, secondly, favours... 

The chemoselectivity of bromination going through bromocarbocations (highly conjugated olefins and also gem-alkenes ) is 100 % in favour of methanol, a nucleophile stronger than bromide ions. However, when the intermediates are bromonium ions, the chemoselectivity is poor. Branched substituents seem to favour the dibromide over the solvent-incorporated adduct, although the bromide ion is considered to be a bulkier nucleophile than methanol. 

Reversible formation of ionic intermediates in halogenated solvents has been suggested to be due to the weakly nucleophilic character of the counteranion, the tribromide ion, which should dissociate into nucleophilic bromide and free bromine before reacting with the bromonium ion (refs. 11,25,26). In order to check this hypothesis the product distribution of the c/s-stilbene bromination in chloroform was investigated (ref. 27). In the latter solvent the formation constant of Br3 is considerably lower than in DCE, Kf = 2.77 (0.13) x 10 against > 2 x 107 M 1. (ref. 28). As a consequence, at 10 3 M [Br2] relevant amounts of bromide ions are present as counteranion of the bromonium intermediate. Nevertheless, the same trend for the isomerization of cis- to rran -stilbene, as well as an increase of... 

The mechanism consists of two successive nucleophilic substitutions, with the tertiary amine as the first nucleophile and the liberated bromide ion as the second ... 

A variety of reagents can function as the electrophile E+ in the general mechanism. The most useful synthetic procedures for preparation of halides are based on the halogens, positive halogens sources, and diethyl azodicarboxylate. A 1 1 adduct formed from triphenylphosphine and bromine converts alcohols to bromides.15 The alcohol displaces bromide ion from the pentavalent adduct, giving an alkoxyphosphonium intermediate. The phosphonium ion intermediate then undergoes nucleophilic attack by bromide ion, forming triphenylphosphine oxide. 

The bridging by bromine prevents rotation about the remaining bond and back-side nucleophilic opening of the bromonium ion by bromide ion leads to the observed anti addition. Direct evidence for the existence of bromonium ions has been obtained from NMR measurements.31 A bromonium ion salt (with Br3 as the counterion) has been isolated from the reaction of bromine with the very hindered alkene adamantylide-neadamantane.32... 

The acetoxy group is introduced exclusively at the benzylic carbon. This is in accord with the intermediate being a weakly bridged species or a benzylic cation. The addition of bromide salts to the reaction mixture diminishes the amount of acetoxy compound formed by shifting the competition for the electrophile in favor of the bromide ion. Chlorination in nucleophilic solvents can also lead to solvent incorporation, as, for example, in the chlorination of 1-phenylpropene in methanol.37... 

This clearly need not necessarily occur under nucleophilic conditions. But we note that in the above case, mesylate, a better leaving group is involved whilst in the present case bromide ion is the leaving group. Does one always get a propellane with the worse... 

The bromide ion acts as a nucleophile while the positive bromine of the bromonium ion acts as a leaving group. 

Nucleophilic attack by the bromide ion causes inversion of the configuration of... 

Then a bromide ion acts as a nucleophile and displaces HOPBr2. 

An Sn2 reaction with a bromide ion acting as the nucleophile produces ethanol and ethyl bromide. 

A mechanistic interpretation is based on the ring-opening principle deduced in the next chapter the very unusual electrophilic attack of bromine at carbonyl oxygen is followed by nucleophilic addition of bromide ion at elevated temperature and ring-opening by transfer of bromine to CljC2. 

Kinetic solvent isotope effect as a measure of electrophilic assistance to bromide ion departure limiting values rate data in ethanol, methanol and their aqueous mixtures using Bentley s TBr scale its decrease corresponds to the involvement of nucleophilic assistance. R = (/caqhtOII//cAcoH)r as a measure of nucleophilic solvent assistance. Model for a limiting bromination mechanism. Ruasse et al. (1991). /Ruasse and Zhang (1984). 9Argile and Ruasse (to be published). Modro et al. (1979). 

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